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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT04801498
Other study ID # STUDY00144620
Secondary ID
Status Recruiting
Phase
First received
Last updated
Start date December 7, 2020
Est. completion date June 30, 2024

Study information

Verified date December 2023
Source University of Kansas Medical Center
Contact Lachlan Moore
Phone 913-588-7630
Email lmoore12@kumc.edu
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

This pilot study is being performed to examine whether epidermal axons are altered in patients taking opioid therapy for chronic non-cancer pain, and if epidermal axonal changes predict heightened pain sensitivity.


Description:

Currently, 1 in 25 adults in the USA regularly uses prescription opioids. Now described as a healthcare crisis, increased prescription opioid use is linked with greater healthcare utilization and its associated negative costs. Prescription opioid use leads to increased mortality due to unintentional overdose, misuse and abuse, transition into illicit opioid use, decreased pain thresholds, and widespread neuropathic pain. In addition, opioid- induced hyperalgesia is a dangerous and paradoxical condition wherein patients on opioids develop increased super- heightened pain. In the USA, the increase in prescription opioid use has followed a similar trajectory of the incidence of overdose due to prescription and illicit opioids. Sadly, even with this drastic escalation in opioid use, there has been no change in the rate or severity of chronic pain conditions. Quantitative analysis of cutaneous innervation of the epidermis provides an indication of the health of peripheral sensory axons. Studies in various pain conditions (e.g., painful diabetic neuropathy, painful chemotherapy-induced neuropathy, and fibromyalgia) suggest changes in epidermal innervation may underlie pain in the feet and hands. Our preclinical studies reveal that changes in epidermal axons play a key role in the development of pain. Here, we postulate that chronic opioid use in patients with chronic pain due to non- cancer conditions 1) contributes to detrimental changes in epidermal axons, 2) works against pain-relieving actions of opioids to reduce pain, and 3) is possibly linked to opioid-induced hyperalgesia. Our short-term goals are to determine if epidermal axons are altered in patients taking opioid therapy for chronic non-cancer pain, and if epidermal axonal changes predict heightened pain sensitivity. This pilot study will test whether changes in epidermal axons are "dose-dependent" in patients taking low-dose, moderate-dose, or high-dose opioid therapy. Our long-term goals will determine whether dose-reduction or cessation of opioids can reverse axonal changes, or whether these adverse chances can be prevented with other medications. Our central hypothesis is that patients on opioid therapy for chronic non-cancer pain will exhibit elevated epidermal axon densities, and these elevations are accompanied with hyperalgesia and allodynia. Aim 1: Do patients on long-term opioid therapy have abnormal intraepidermal nerve fiber (IENF) density? We hypothesize that patients taking chronic opioids for non-cancer pain conditions will exhibit abnormal epidermal nerve fiber density compared to chronic pain patients not taking opioid therapy and healthy controls. We will recruit 20 patients with chronic pain due to non-cancer conditions on opioid therapy, 20 patients with chronic pain not taking opioid therapy, and 20 healthy controls and perform a skin biopsy on the ankle. The skin biopsy will then be assessed to ascertain IENF density and compared to normative density values for sex and age. Next, we will compare quantitative measurements of IENF density to total daily oral morphine equivalents (OME) taken by the patients. We hypothesize that higher daily opioid consumption will correlate with abnormalities in epidermal innervation. Aim 2: Do patients on long-term opioid therapy have heightened cutaneous pain sensitivity that correlates with IENF density? We will perform quantitative sensory testing (QST) in all patient cohorts to objectively assess pain sensitivity. Patients will undergo QST for pressure pain threshold, temporal summation, and conditioned pain modulation. We will determine whether heightened pain sensitivity, as evidenced by reduced pressure pain thresholds, increased temporal summation, and reduced conditioned pain modulation, is associated with altered IENF from skin biopsies. We hypothesize that heightened pain sensitivity will correlate with reductions in epidermal innervation and that higher daily opioid consumption in chronic pain patients will correlate with abnormalities in epidermal innervation and altered QST parameters.


Recruitment information / eligibility

Status Recruiting
Enrollment 60
Est. completion date June 30, 2024
Est. primary completion date June 30, 2024
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria: Healthy/All: - Informed consent provided by the participant - Able to read and speak in English - Age 18 to 65 years - Likely to participate in all scheduled evaluations and study procedures IF they are a Chronic Non-Cancer Patients who do NOT take opioid medication they must meet all of the above criteria as well as: Diagnosis of non-cancer chronic pain syndrome (persistent pain lasting longer than 3 months) IF they are a Chronic Non-Cancer Patients who DO take opioid medication they must meet all of the above criteria as well as: - Chronic daily opioid use for longer than 3 months duration - Stable doses of opioid medications for at least 30 days prior to study visit Exclusion Criteria: - Pregnancy - Prisoner - Current clinically significant cardiac, or neurologic disease - Significant skin disorders in lower extremities - Circulatory insufficiency - Open wounds in lower extremity that may interfere with healing - Lidocaine allergy - Currently taking anticoagulation (e.g., Coumadin, Plavix, etc) - Current litigation for chronic pain - Active psychotic or suicidal symptoms - Current drug or alcohol abuse - Neuropathy in upper extremities (hands specifically, PI discretion). - Current or recent use of artificial fingernails or nail enhancements (last 6 months) - Other diagnoses that are not considered minor/stable (PI discretion) - Current or previous cancer diagnosis - Current or previous chemotherapy treatment - No chronic pain conditions (healthy) - Opioid use in the last year (healthy & non-opioid pts)

Study Design


Related Conditions & MeSH terms


Locations

Country Name City State
United States University of Kansas Health System Kansas City Kansas

Sponsors (1)

Lead Sponsor Collaborator
University of Kansas Medical Center

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary IENFD Intraepidermal Nerve Fiber Density Baseline
Secondary Fibromyalgianess FMness is a measure of pain and co-morbid symptom extensiveness and severity. It is calculated from the 2011 FM Survey27 to derive a continuous metric of CNS pain amplification. Baseline
Secondary Clinical Pain Severity Pain severity and interference will be assessed using the Brief Pain Inventory (BPI). The BPI asks patients to rate their worst, least and average pain intensity (0-10 NRS). Baseline
Secondary Neuropathic Pain Descriptors The PainDETECT is a 9-item measure of sensory descriptors and spatial and temporal characteristics that indicates neuropathic pain Baseline
Secondary Stress The Perceived Stress Scale (PSS) is used to measure levels of stress. Baseline
Secondary Catastrophizing Coping Strategies Questionnaire(CSQ-CAT) will quantify traits associated with pain progression and catastrophizing Baseline
Secondary Physical Functioning The PROMIS short forms will be used for Fatigue, Sleep Disturbance, Sleep-Related Impairment, Physical Function, Anxiety and Depression Baseline
Secondary Sleep Disturbance The PROMIS short forms will be used for Fatigue, Sleep Disturbance, Sleep-Related Impairment, Physical Function, Anxiety and Depression Baseline
Secondary Sleep Related Impairment The PROMIS short forms will be used for Fatigue, Sleep Disturbance, Sleep-Related Impairment, Physical Function, Anxiety and Depression Baseline
Secondary Fatigue The PROMIS short forms will be used for Fatigue, Sleep Disturbance, Sleep-Related Impairment, Physical Function, Anxiety and Depression Baseline
Secondary Anxiety The PROMIS short forms will be used for Fatigue, Sleep Disturbance, Sleep-Related Impairment, Physical Function, Anxiety and Depression Baseline
Secondary Depression The PROMIS short forms will be used for Fatigue, Sleep Disturbance, Sleep-Related Impairment, Physical Function, Anxiety and Depression Baseline
Secondary Impulsivity Using the Kirby Delay Discounting Task, a type of impulsivity can be measured by determining the value participants see in rewards if they are offered at different time points (eg. $25 now OR $60 in 21 days).Impulsivity is a measure of a person's propensity towards reward-based behaviors. Patients in chronic pain and on opioids have been shown to have changes in their reward pathways. Baseline
Secondary Pressure Pain Sensitivity Using the Multimodal Automated Sensory Testing (MAST) System, a computerized QST device, an ascending series of 5-s duration stimuli at 25-s intervals will be delivered beginning at 0.50 kg/cm2 and increasing in 0.50 kg/cm2 intervals up to tolerance or a maximum of 10 kg/cm2. Pain intensity and pressure pain threshold will be determined. Baseline
Secondary Conditioned Pain Modulation (CPM) CPM is a measure of the integrity of descending analgesic pathways. CPM will be evaluated using two MAST pressure actuators positioned on opposite thumbnails. A reduction in test stimulus rating by conditioning stimulation implies functional (inhibitory) CPM. Baseline
Secondary Temporal Summation (TS) TS is the perceived increase in pain intensity to repeated stimulation at a constant stimulus intensity and is reflective of CNS sensitization. A 256 mN pinprick stimulus (MRC Systems, Heidelberg, Germany) will be applied once to the forearm or hand, followed by a train of 10 identical stimuli (1 Hz). The series will be repeated three times. Participants report the pain intensity and the mean pain rating is used to calculate a wind-up ratio (WUR); a WUR >1 indicates temporal summation. Baseline
Secondary Pain genetics A number of genes will be analyzed that have previously been studied for their role in pain sensitivity as well as susceptibility to the development of chronic idiopathic low back pain. Subsequent analysis will be performed based on research findings and other published data. Baseline
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